Frontiers in Immunology (Dec 2022)

Markers of blood-brain barrier disruption increase early and persistently in COVID-19 patients with neurological manifestations

  • Valentina Bonetto,
  • Laura Pasetto,
  • Ilaria Lisi,
  • Marco Carbonara,
  • Rosalia Zangari,
  • Erica Ferrari,
  • Veronica Punzi,
  • Silvia Luotti,
  • Nicola Bottino,
  • Bruno Biagianti,
  • Cristina Moglia,
  • Cristina Moglia,
  • Giuseppe Fuda,
  • Roberta Gualtierotti,
  • Francesco Blasi,
  • Francesco Blasi,
  • Ciro Canetta,
  • Nicola Montano,
  • Mauro Tettamanti,
  • Giorgia Camera,
  • Maria Grimoldi,
  • Giulia Negro,
  • Nicola Rifino,
  • Andrea Calvo,
  • Andrea Calvo,
  • Paolo Brambilla,
  • Paolo Brambilla,
  • Francesco Biroli,
  • Alessandra Bandera,
  • Alessandra Bandera,
  • Alessandro Nobili,
  • Nino Stocchetti,
  • Nino Stocchetti,
  • Maria Sessa,
  • Elisa R. Zanier

DOI
https://doi.org/10.3389/fimmu.2022.1070379
Journal volume & issue
Vol. 13

Abstract

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BackgroundCoronavirus disease 2019 (COVID-19) caused by SARS-CoV-2 infection is associated with disorders affecting the peripheral and the central nervous system. A high number of patients develop post-COVID-19 syndrome with the persistence of a large spectrum of symptoms, including neurological, beyond 4 weeks after infection. Several potential mechanisms in the acute phase have been hypothesized, including damage of the blood-brain-barrier (BBB). We tested weather markers of BBB damage in association with markers of brain injury and systemic inflammation may help in identifying a blood signature for disease severity and neurological complications.MethodsBlood biomarkers of BBB disruption (MMP-9, GFAP), neuronal damage (NFL) and systemic inflammation (PPIA, IL-10, TNFα) were measured in two COVID-19 patient cohorts with high disease severity (ICUCovid; n=79) and with neurological complications (NeuroCovid; n=78), and in two control groups free from COVID-19 history, healthy subjects (n=20) and patients with amyotrophic lateral sclerosis (ALS; n=51). Samples from COVID-19 patients were collected during the first and the second wave of COVID-19 pandemic in Lombardy, Italy. Evaluations were done at acute and chronic phases of the COVID-19 infection.ResultsBlood biomarkers of BBB disruption and neuronal damage are high in COVID-19 patients with levels similar to or higher than ALS. NeuroCovid patients display lower levels of the cytokine storm inducer PPIA but higher levels of MMP-9 than ICUCovid patients. There was evidence of different temporal dynamics in ICUCovid compared to NeuroCovid patients with PPIA and IL-10 showing the highest levels in ICUCovid patients at acute phase. On the contrary, MMP-9 was higher at acute phase in NeuroCovid patients, with a severity dependency in the long-term. We also found a clear severity dependency of NFL and GFAP levels, with deceased patients showing the highest levels.DiscussionThe overall picture points to an increased risk for neurological complications in association with high levels of biomarkers of BBB disruption. Our observations may provide hints for therapeutic approaches mitigating BBB disruption to reduce the neurological damage in the acute phase and potential dysfunction in the long-term.

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